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Targeting the local tumor microenvironment with vaccinia virus expressing B7.1 for the treatment of melanoma

机译:用表达B7.1的牛痘病毒靶向局部肿瘤微环境以治疗黑色素瘤

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摘要

Immunotherapy for the treatment of metastatic melanoma remains a major clinical challenge. The melanoma microenvironment may lead to local T cell tolerance in part through downregulation of costimulatory molecules, such as B7.1 (CD80). We report the results from the first clinical trial, to our knowledge, using a recombinant vaccinia virus expressing B7.1 (rV-B7.1) for monthly intralesional vaccination of accessible melanoma lesions. A standard 2-dose–escalation phase I clinical trial was conducted with 12 patients. The approach was well tolerated with only low-grade fever, myalgias, and fatigue reported and 2 patients experiencing vitiligo. An objective partial response was observed in 1 patient and disease stabilization in 2 patients, 1 of whom is alive without disease 59 months following vaccination. All patients demonstrated an increase in postvaccination antibody and T cell responses against vaccinia virus. Systemic immunity was tested in HLA-A*0201 patients who demonstrated an increased frequency of gp100 and T cells specific to melanoma antigen recognized by T cells 1 (MART-1), also known as Melan-A, by ELISPOT assay following local rV-B7.1 vaccination. Local immunity was evaluated by quantitative real-time RT-PCR, which suggested that tumor regression was associated with increased expression of CD8 and IFN-γ. The local delivery of vaccinia virus expressing B7.1 was well tolerated and represents an innovative strategy for altering the local tumor microenvironment in patients with melanoma.
机译:免疫疗法治疗转移性黑色素瘤仍然是主要的临床挑战。黑色素瘤微环境可能部分通过共刺激分子(例如B7.1(CD80))的下调而导致局部T细胞耐受。据我们所知,我们使用表达B7.1(rV-B7.1)的重组牛痘病毒每月进行一次可及的黑色素瘤病变的病灶内疫苗接种,报告了第一项临床试验的结果。一项标准的2剂量升级I期临床试验针对12位患者进行。仅对低烧,肌痛和疲乏有报道,并且有2名白癜风患者对该方法耐受良好。在1名患者中观察到客观的部分反应,在2名患者中病情稳定,其中1名在接种疫苗59个月后还没有疾病存活。所有患者均显示出针对牛痘病毒的疫苗接种后抗体和T细胞应答增加。在HLA-A * 0201患者中进行了全身免疫测试,这些患者通过局部rV-后通过ELISPOT分析证实了被T细胞1(MART-1)识别的黑色素瘤抗原特异的gp100和T细胞(也称为Melan-A)的频率增加。 B7.1疫苗接种。通过定量实时RT-PCR评估局部免疫,这表明肿瘤消退与CD8和IFN-γ的表达增加有关。表达B7.1的痘苗病毒的局部递送具有良好的耐受性,代表了改变黑素瘤患者局部肿瘤微环境的创新策略。

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